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Characterization of beta2 (CD18) integrin phosphorylation in phorbol ester-activated T lymphocytes.

机译:佛波酯活化的T淋巴细胞中β2(CD18)整合素磷酸化的特征。

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摘要

Integrins are transmembrane proteins involved in cell-cell and cell-extracellular-matrix interactions. The affinity and avidity of integrins for their ligands change in response to cytoplasmic signals. This 'inside-out' activation has been reported to occur also with beta2 integrins (CD18). The beta2 integrin subunit has previously been shown to become phosphorylated in T lymphocytes on cytoplasmic serine and the functionally important threonine residues after treatment with phorbol esters or on triggering of T-cell receptors. We have now characterized the phosphorylation of beta2 integrins in T-cells in more detail. When T-cells were activated by phorbol esters the phosphorylation was mainly on Ser756. After inhibition of serine/threonine phosphatases, phosphorylation was also found in two of the threonine residues in the threonine triplet 758-760 of the beta2 cytoplasmic domain. Activation of T-cells by phorbol esters resulted in phosphorylation in only approx. 10% of the integrin molecules. Okadaic acid increased this phosphorylation to approx. 30% of the beta2 molecules, assuming three phosphorylation sites. This indicates that a strong dynamic phosphorylation exists in serine and threonine residues of the beta2 integrins.
机译:整联蛋白是参与细胞-细胞和细胞-细胞外-基质相互作用的跨膜蛋白。整联蛋白对其配体的亲和力和亲合力响应细胞质信号而改变。据报道,这种“由内而外”的激活也与beta2整合素(CD18)一起发生。以前已经证明,在使用佛波醇酯处理或触发T细胞受体后,β2整合素亚基在胞浆丝氨酸和功能重要的苏氨酸残基的T淋巴细胞中被磷酸化。现在我们已经更详细地描述了T细胞中β2整合素的磷酸化。当T细胞被佛波酯活化时,磷酸化主要在Ser756上。在抑制丝氨酸/苏氨酸磷酸酶后,在β2细胞质结构域的苏氨酸三联体758-760中的两个苏氨酸残基中也发现了磷酸化。佛波酯对T细胞的激活仅导致约20%的磷酸化。整联蛋白分子的10%。冈田酸将这种磷酸化作用提高至约。假设三个磷酸化位点,其中30%的beta2分子。这表明在β2整联蛋白的丝氨酸和苏氨酸残基中存在强烈的动态磷酸化。

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